The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity

The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity

Quinolones are broad-spectrum synthetic antibacterial drugs first obtained during the synthesis of chloroquine. Nalidixic acid, the prototype of quinolones, first became available for clinical consumption in 1962 and was used mainly for urinary tract infections caused by Escherichia coli and other p...

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Main Authors: Abdul Naeem, Syed Lal Badshah, Mairman Muska, Nasir Ahmad, Khalid Khan
Format: Article
Language:English
Published: MDPI AG 2016-03-01
Series:Molecules
Subjects:
quinolones
analogues
gyrase
topoisomerase IV
resistance
Online Access:http://www.mdpi.com/1420-3049/21/4/268
id doaj-d186402405db4ebfbb95c344fe14a4d5
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spelling doaj-d186402405db4ebfbb95c344fe14a4d52020-11-24T21:27:18ZengMDPI AGMolecules1420-30492016-03-0121426810.3390/molecules21040268molecules21040268The Current Case of Quinolones: Synthetic Approaches and Antibacterial ActivityAbdul Naeem0Syed Lal Badshah1Mairman Muska2Nasir Ahmad3Khalid Khan4National Center of Excellence in Physical Chemistry, University of Peshawar, Peshawar, Khyber Pukhtoonkhwa 25120, PakistanNational Center of Excellence in Physical Chemistry, University of Peshawar, Peshawar, Khyber Pukhtoonkhwa 25120, PakistanNational Center of Excellence in Physical Chemistry, University of Peshawar, Peshawar, Khyber Pukhtoonkhwa 25120, PakistanDepartment of Chemistry, Islamia College University Peshawar, Peshawar, Khyber Pukhtoonkhwa 25120, PakistanDepartment of Chemistry, Islamia College University Peshawar, Peshawar, Khyber Pukhtoonkhwa 25120, PakistanQuinolones are broad-spectrum synthetic antibacterial drugs first obtained during the synthesis of chloroquine. Nalidixic acid, the prototype of quinolones, first became available for clinical consumption in 1962 and was used mainly for urinary tract infections caused by Escherichia coli and other pathogenic Gram-negative bacteria. Recently, significant work has been carried out to synthesize novel quinolone analogues with enhanced activity and potential usage for the treatment of different bacterial diseases. These novel analogues are made by substitution at different sites—the variation at the C-6 and C-8 positions gives more effective drugs. Substitution of a fluorine atom at the C-6 position produces fluroquinolones, which account for a large proportion of the quinolones in clinical use. Among others, substitution of piperazine or methylpiperazine, pyrrolidinyl and piperidinyl rings also yields effective analogues. A total of twenty six analogues are reported in this review. The targets of quinolones are two bacterial enzymes of the class II topoisomerase family, namely gyrase and topoisomerase IV. Quinolones increase the concentration of drug-enzyme-DNA cleavage complexes and convert them into cellular toxins; as a result they are bactericidal. High bioavailability, relative low toxicity and favorable pharmacokinetics have resulted in the clinical success of fluoroquinolones and quinolones. Due to these superior properties, quinolones have been extensively utilized and this increased usage has resulted in some quinolone-resistant bacterial strains. Bacteria become resistant to quinolones by three mechanisms: (1) mutation in the target site (gyrase and/or topoisomerase IV) of quinolones; (2) plasmid-mediated resistance; and (3) chromosome-mediated quinolone resistance. In plasmid-mediated resistance, the efflux of quinolones is increased along with a decrease in the interaction of the drug with gyrase (topoisomerase IV). In the case of chromosome-mediated quinolone resistance, there is a decrease in the influx of the drug into the cell.http://www.mdpi.com/1420-3049/21/4/268quinolonesanaloguesgyrasetopoisomerase IVresistance
collection DOAJ
language English
format Article
sources DOAJ
author Abdul Naeem
Syed Lal Badshah
Mairman Muska
Nasir Ahmad
Khalid Khan
spellingShingle Abdul Naeem
Syed Lal Badshah
Mairman Muska
Nasir Ahmad
Khalid Khan
The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity
Molecules
quinolones
analogues
gyrase
topoisomerase IV
resistance
author_facet Abdul Naeem
Syed Lal Badshah
Mairman Muska
Nasir Ahmad
Khalid Khan
author_sort Abdul Naeem
title The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity
title_short The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity
title_full The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity
title_fullStr The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity
title_full_unstemmed The Current Case of Quinolones: Synthetic Approaches and Antibacterial Activity
title_sort current case of quinolones: synthetic approaches and antibacterial activity
publisher MDPI AG
series Molecules
issn 1420-3049
publishDate 2016-03-01
description Quinolones are broad-spectrum synthetic antibacterial drugs first obtained during the synthesis of chloroquine. Nalidixic acid, the prototype of quinolones, first became available for clinical consumption in 1962 and was used mainly for urinary tract infections caused by Escherichia coli and other pathogenic Gram-negative bacteria. Recently, significant work has been carried out to synthesize novel quinolone analogues with enhanced activity and potential usage for the treatment of different bacterial diseases. These novel analogues are made by substitution at different sites—the variation at the C-6 and C-8 positions gives more effective drugs. Substitution of a fluorine atom at the C-6 position produces fluroquinolones, which account for a large proportion of the quinolones in clinical use. Among others, substitution of piperazine or methylpiperazine, pyrrolidinyl and piperidinyl rings also yields effective analogues. A total of twenty six analogues are reported in this review. The targets of quinolones are two bacterial enzymes of the class II topoisomerase family, namely gyrase and topoisomerase IV. Quinolones increase the concentration of drug-enzyme-DNA cleavage complexes and convert them into cellular toxins; as a result they are bactericidal. High bioavailability, relative low toxicity and favorable pharmacokinetics have resulted in the clinical success of fluoroquinolones and quinolones. Due to these superior properties, quinolones have been extensively utilized and this increased usage has resulted in some quinolone-resistant bacterial strains. Bacteria become resistant to quinolones by three mechanisms: (1) mutation in the target site (gyrase and/or topoisomerase IV) of quinolones; (2) plasmid-mediated resistance; and (3) chromosome-mediated quinolone resistance. In plasmid-mediated resistance, the efflux of quinolones is increased along with a decrease in the interaction of the drug with gyrase (topoisomerase IV). In the case of chromosome-mediated quinolone resistance, there is a decrease in the influx of the drug into the cell.
topic quinolones
analogues
gyrase
topoisomerase IV
resistance
url http://www.mdpi.com/1420-3049/21/4/268
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